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Pharmacology of drugs used in bronchial asthma & COPD

Pharmacology of drugs used in bronchial asthma & COPD. By Prof. Hanan Hagar. Disorders of Respiratory Function Main disorders of the respiratory system are : 1. Bronchial asthma 2. Cough 3. Allergic rhinitis 4. Chronic obstructive pulmonary disease (COPD, also called emphysema). Asthma

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Pharmacology of drugs used in bronchial asthma & COPD

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  1. Pharmacology of drugs used inbronchial asthma & COPD By Prof. Hanan Hagar

  2. Disorders of Respiratory Function Main disorders of the respiratory system are : 1. Bronchial asthma 2. Cough 3. Allergic rhinitis 4. Chronic obstructive pulmonary disease (COPD, also called emphysema)

  3. Asthma Asthma is a chronic inflammatory disorder of bronchial airways that result in airway obstruction in response to external stimuli (as pollen grains, cold air and tobacco smoke).

  4. Characters of airways in asthmatic patients : • Airway hyper-reactivity: abnormal sensitivity of • the airways to wide range of external stimuli. • Inflammation • Swelling • Thick mucus production. • Bronchospasm (constriction of the bronchial muscles).

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  6. Symptoms of asthma Asthma produces recurrent episodic attack of • Acute bronchoconstriction • Shortness of breath • Chest tightness • Wheezing • Rapid respiration • Cough Symptoms can happen each time the airways are irritated by inhaled irritants or allergens.

  7. Causes • Infection • Emotional conditions • Stress • Exercise • Pets • Seasonal changes • Some drugs as aspirin, β bockers

  8. Airways Innervations Afferent nerves (sensory) • Irritant receptors in upper airways. • C-fiber receptors in lower airways. Stimulated by : Exogenous chemicals Physical stimuli (cold air) Endogenous inflammatory mediators

  9. Efferent nerves (motor) • Parasympathetic supply M3 receptors in smooth muscles and glands. • No sympathetic supplybut B2 receptors in smooth muscles and glands

  10. Aims of anti asthmatic drugs: • To relieve acute episodic attacks of asthma (bronchodilators, quick relief medications). • To reduce the frequency of attacks, and • nocturnal awakenings (anti-inflammatory drugs, prophylactic or control therapy ).

  11. Bronchodilators (Quick relief medications) treat acute episodic attack of asthma • Short acting 2-agonists • Antimuscarinics • Xanthine preparations Anti-inflammatory Agents (control medications or prophylactic therapy) • reduce the frequency of attacks • Corticosteroids • Mast cell stabilizers • Leukotrienes antagonists • Anti-IgE monoclonal antibody • Long acting ß2-agonists Anti asthmatic drugs

  12. Anti asthmatic drugs Bronchodilators : (Quick relief medications) are used to relieve acute attack of bronchoconstriction 1. 2 - adrenoreceptor agonists 2. Antimuscarinics 3. Xanthine preparations

  13. Sympathomimetics - adrenoceptor agonists Mechanism of Action • direct 2stimulation  stimulate adenyl cyclase  Increase cAMP  bronchodilation • Inhibit mediators release from mast cells. • Increase mucus clearance by (increasing ciliary activity).

  14. Classification of  agonists • Non selective  agonists: epinephrine - isoprenaline • Selective 2 – agonists (Preferable). Salbutamol (albuterol) Terbutaline Salmeterol Formeterol

  15. Non selective -agonists. Epinephrine • Potent bronchodilator • rapid action (maximum effect within 15 min). • S.C. or by inhalation (aerosol or nebulizer). • Has short duration of action (60-90 min) • Drug of choice for acute anaphylaxis (hypersensitivity reactions).

  16. Nebulizer Inhaler

  17. Disadvantages • Not effective orally. • Hyperglycemia • CVS side effects: tachycardia, arrhythmia, hypertension • Skeletal muscle tremor • Not suitable for asthmatic patients with hypertension or heart failure. Contraindication: CVS patients, diabetic patients

  18. Selective 2 –agonists • drugs of choice for acute attack of asthma • Are mainly given by inhalation (metered dose inhaler or nebulizer). • Can be given orally, parenterally. • Short acting ß2 agonists e.g. salbutamol, terbutaline • Long acting ß2 agonists e.g. salmeterol, formeterol

  19. Short acting ß2 agonists Salbutamol, inhalation, orally, i.v. Terbutaline, inhalation, orally, s.c. • Have rapid onset of action (15-30 min). • short duration of action (4-6 hr) • used for symptomatic treatment of acute episodic attack of asthma.

  20. Long acting selective ß2 agonists • Salmeterol & formoterol: • Long acting bronchodilators (12 hours) • have high lipid solubility (creates depot effect) • are given by inhalation • are not used to relieve acute episodes of asthma • used for nocturnal asthma (long acting relievers). • combined with inhaled corticosteroids to control asthma (decreases the number and severity of asthma attacks).

  21. Advantages of ß2 agonists • Minimal CVS side effects • suitable for asthmatic patients with hypertension or heart failure. Disadvantages of ß2 agonists • Skeletal muscle tremors. • Nervousness • Tolerance (B-receptors down regulation). • Tachycardia over dose (B1-stimulation).

  22. Muscarinic antagonists Ipratropium – Tiotropium • Act by blocking muscarinic receptors. • Given by aerosol inhalation • Quaternary derivatives of atropine • Does not diffuse into the blood • Do not enter CNS, minimal systemic side effects. • Delayed onset of action • Ipratropium has short duration of action 3-5 hr • Tiotropium has longer duration of action (24 h).

  23. Pharmacodynamics • are short-acting bronchodilator. • Inhibit bronchoconstriction and mucus secretion • Less effective than β2-agonists. • No anti-inflammatory action Uses • Main choice in chronic obstructive pulmonary diseases (COPD). • In acute severe asthma combined with β2-agonists & steroids.

  24. Methylxanthines • Theophylline - aminophylline Mechanism of Action • are phosphodiestrase inhibitors •  cAMP  bronchodilation • Adenosine receptors antagonists (A1) • Increase diaphragmatic contraction • Stabilization of mast cell membrane

  25. ATP Bronchodilation Adenyl cyclase B-agonists cAMP Bronchial tree Phosphodiesterase Theophylline Adenosine Bronchoconstriction 3,5,AMP

  26. Pharmacological effects : • Bronchial muscle relaxation • contraction of diaphragm improve ventilation CVS: ↑ heart rate, ↑ force of contraction GIT: ↑ gastric acid secretions Kidney: ↑renal blood flow, weak diuretic action CNS stimulation * stimulant effect on respiratory center. * decrease fatigue & elevate mood. * overdose (tremors, nervousness, insomnia, convulsion)

  27. Pharmacokinetics • metabolized by Cyt P450 enzymes in liver • T ½= 8 hours • has many drug interactions • Enzyme inducers: as phenobarbitone-rifampicin → ↑metabolism of theophylline → ↓ T ½. • Enzyme inhibitors: as erythromycin→ ↓ metabolism of theophylline → ↑T ½.

  28. Uses • Second line drug in asthma (theophylline) • For status asthmatics (aminophylline, is given asslow infusion). Side Effects • Low therapeutic indexnarrow safety margin monitoring of theophylline blood level is necessary. • CVS effects:hypotension, arrhythmia. • GIT effects:nausea & vomiting • CNS side effects:tremors, nervousness, insomnia, convulsion

  29. Anti - inflammatory agents include: • Glucocorticoids • Leukotrienes antagonists • Mast cell stabilizers • Anti-IgE monoclonal antibody (omalizumab)

  30. Anti - inflammatory Agents: (control medications / prophylactic therapy) reducethe number of inflammatory cells in the airways and prevent blood vessels from leaking fluid into the airway tissues. By reducing inflammation, they reduce the spasm of airways & bronchial hyper-reactivity.

  31. Glucocorticoids Mechanism of action • Inhibition of phospholipase A2 • ↓ prostaglandin and leukotrienes • ↓ Number of inflammatory cells in airways. • Mast cell stabilization →↓ histamine release. • ↓ capillary permeability and mucosal edema. • Inhibition of antigen-antibody reaction. • Upregulate β2 receptors (have additive effect to B2 agonists).

  32. Pharmacological actions of glucocorticoids Anti-inflammatory actions Immunosuppressant effects Metabolic effects Hyperglycemia ↑ protein catabolism, ↓ protein anabolism Stimulation oflipolysis- fat redistribution Mineralocorticoid effects: sodium/fluid retention Increase potassium excretion (hypokalemia) Increase blood volume (hypertension)

  33. Behavioral changes: depression Bone loss (osteoporosis) due to Inhibit bone formation ↓ calcium absorption.

  34. Routes of administration • Inhalation: e.g. Budesonide & Fluticasone, beclometasone • Given by inhalation, given by metered-dose inhaler • Have first pass metabolism • Best choice in asthma, less side effects • Orally:Prednisone, methyl prednisolone • Injection:Hydrocortisone, dexamethasone

  35. Glucocorticoids in asthma • Are not bronchodilators • Reduce bronchial inflammation • Reduce bronchial hyper-reactivity to stimuli • Have delayed onset of action (effect usually attained after 2-4 weeks). • Maximum action at 9-12 months. • Given as prophylactic medications, used alone or combined with beta-agonists. • Effective in allergic, exercise, antigen and irritant-induced asthma,

  36. Systemic corticosteroids are reserved for: • Status asthmaticus (i.v.). Inhaled steroids should be considered for adults, children with any of the following features • using inhaled β2 agonists three times/week • symptomatic three times/ week or more; • or waking one night/week.

  37. Clinical Uses of glucocorticoids Treatment of inflammatory disorders (asthma, rheumatoid arthritis). Treatment of autoimmune disorders (ulcerative colitis, psoriasis) and after organ or bone marrow transplantation. Antiemetics in cancer chemotherapy

  38. Side effects due to systemic corticosteroids • Adrenal suppression • Growth retardation in children • Osteoporosis • Fluid retention, weight gain, hypertension • Hyperglycemia • Susceptibility to infections • Glaucoma • Cataract • Fat distribution, wasting of the muscles • Psychosis

  39. Inhalation has very less side effects: • Oropharyngeal candidiasis (thrush). • Dysphonia (voice hoarseness). Withdrawal • Abrupt stop of corticosteroids should be avoided and dose should be tapered (adrenal insufficiency syndrome).

  40. Mast cell stabilizers e.g. Cromolyn (cromoglycate) - Nedocromil • act by stabilization of mast cell membrane. • given by inhalation (aerosol, microfine powder, nebulizer). • Have poor oral absorption (10%)

  41. Pharmacodynamics • areNotbronchodilators • Not effective in acute attack of asthma. • Prophylactic anti-inflammatory drug • Reduce bronchial hyper-reactivity. • Effective in exercise, antigen and irritant-induced asthma. • Children respond better than adults

  42. Uses • Prophylactic therapy in asthma especially in children. • Allergic rhinitis. • Conjunctivitis. Side effects • Bitter taste • minor upper respiratory tract irritation (burning sensation, nasal congestion)

  43. Leukotrienes antagonists Leukotrienes • produced by the action of 5-lipoxygenase on arachidonic acid. • Synthesized by inflammatory cells found in the airways (eosinophils, macrophages, mast cells). • Leukotriene B4: chemotaxis of neutrophils • Cysteinyl leukotrienes C4, D4 & E4: • bronchoconstriction •  increase bronchial hyper-reactivity • mucosal edema, mucus hyper-secretion

  44. Leukotriene receptor antagonists e.g. zafirlukast, montelukast, pranlukast • are selective, reversible antagonists of cysteinyl leukotriene receptors (CysLT1receptors). • Taken orally. • Are bronchodilators • Have anti-inflammatory action • Less effective than inhaled corticosteroids • Have glucocorticoids sparing effect (potentiate corticosteroid actions).

  45. Uses of leukotriene receptor antagonists • Are not effective to relieve acute attack of asthma. • Prophylaxis of mild to moderate asthma. • Aspirin-induced asthma • Antigen and exercise-induced asthma • Can be combined with glucocorticoids (additive effects, low dose of glucocorticoids can be used). Side effects: Elevation of liver enzymes, headache, dyspepsia

  46. Omalizumab • is a monoclonal antibody directed against human IgE. • prevents IgE binding with its receptors on mast cells & basophiles. • ↓ release of allergic mediators. • used for treatment of allergic asthma. • Expensive-not first line therapy.

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